Inflammation, Autoimmunity and Neurodegenerative Diseases, Therapeutics and Beyond

Neurodegenerative disease (ND) incidence has recently increased due to improved life expectancy. Alzheimer's (AD) or Parkinson's disease (PD) are the most prevalent NDs. Both diseases are poly genetic, multifactorial and heterogenous. Preventive medicine, a healthy diet, exercise, and controlling comorbidities may delay the onset. After the diseases are diagnosed, therapy is needed to slow progression. Recent studies show that local, peripheral and age-related inflammation accelerates NDs' onset and progression. Patients with autoimmune disorders like inflammatory bowel disease (IBD) could be at higher risk of developing AD or PD. However, no increase in ND incidence has been reported if the patients are adequately diagnosed and treated. Autoantibodies against abnormal tau, β amyloid and α- synuclein have been encountered in AD and PD and may be protective. This discovery led to the proposal of immune-based therapies for AD and PD involving monoclonal antibodies, immunization/vaccines, pro-inflammatory cytokine inhibition and anti-inflammatory cytokine addition. All the different approaches have been analysed here. Future perspectives on new therapeutic strategies for both disorders are concisely examined.


INTRODUCTION 1.General Overview
Neurodegeneration refers to the progressive deterioration and loss of function of neurons.Neurodegenerative diseases (ND) include Alzheimer's disease (AD), Amyotrophic lateral sclerosis (ALS), Friedreich ataxia, Frontotemporal lobular degeneration (FTLD), Huntington's disease (HD), Lewy body dementia, Multiple Sclerosis (MS), Parkinson's disease (PD), and Spinal muscular atrophy (SMA).All NDs have different origins.Genetic involvement in several NDs has been studied for years [1].HD and ALS are primary examples.HD is a progressive brain disorder caused by a single defective gene on chromosome 4 that codifies for the protein huntingtin.The disease generally manifests between 30 and 50 years [2].ALS is a neurodegenerative disease that affects motor neurons.Around 60% of ALS patients have a genetic correlation with the disease.The genes associated with ALS *Address correspondence to this author at the Institute of Molecular and Translational Medicine, Faculty of Medicine and Dentistry, The Czech Advanced Technology and Research Institute (Catrin), Palacky University, Hněvotínská 1333/5, 779 00 Olomouc, The Czech Republic; E-mails: sanctisj@gmail.com;juanbautista.desanctis@upol.cz1875-6190/24 are: 1) superoxide dismutase 1 (SOD1), 2) TAR DNA binding protein (TDP-53), 3) fused in sarcoma (FUS) and 4) chromosome 9 open reading frame 72 (C9orf72) [3].Some other genes have been recently discovered.MS is an autoimmune neurodegenerative disease associated with demyelination, inflammation and irreversible axonal loss [4].Myelin is the target antigen, and demyelination results in axonal loss, the primary cause of irreversible neurological disability in MS [4][5][6].MS's inflammatory aspects are unique compared to other NDs [4][5][6].The immunogenetic analysis of MS patients has revealed a link between the polymorphisms of HLA [6].HLA DRB1*15:01 and HLA DRB1*04 with younger age of onset, HLA DRB1*03 could be linked to pediatric forms, and MHLA-B*44:02 appears to be associated with less cortical atrophy and fewer MRI brain lesions [6].Since AD and PD are the most common neurodegenerative disorders (4% of individuals over 65 and 1% of people over the age of 60, respectively), the review will focus mainly on these diseases [7,8].Genetic predisposition, malnutrition, the excessive use of legal and non-legal drugs, comorbidities and other environmental events may increase the prevalence and earlier onset of NDs.The central nervous system (CNS) is highly regulated and guarded by physical barriers and specialised cells.The blood-brain barrier (BBB) and blood-spinal cord barrier (BSCB) are not physical barriers, but cells (pericytes) that heavily restrict the flow of molecules by tightening blood capillaries and the secreting VE-cadherin and P-glycoprotein [22].These physical barriers can be more permeable with age [23].The main difference between the BBB and the BSCB is the size of the zonula occludens (multiprotein complexes that prevent leakage of solutes and water between the epithelial cells) and the number of pericytes, allowing a more extensive range of molecules to pass through the barrier in BSCB.It is, therefore, assumed that the spinal cord may be more susceptible to inflammatory insults than the brain [24].In neuroinflammatory disorders like PD, AD, MS, stroke/ ischemia, epilepsy, traumatic brain injury (TBI) and spinal cord injury (SCI), there is a dysfunction of the BBB and BSCB [24].This dysfunction is characterised by phenotypically altered endothelial cells and decreased tight junction proteins facilitating leukocyte migration [24].Chronic inflammation or acute injuries can disrupt the integrity of the BBB, leading to the infiltration of systemic immune cells and mediators, further exacerbating a proinflammatory environment in the CNS [24].Incomplete or impaired responses observed in ageing can be linked to an increased risk of developing neurodegenerative diseases [25].Innate immune responses recruit cells of the adaptive immune system by secreting various cytokines and chemokines that prompt local cells to express adhesion molecules on the BBB and costimulatory molecules on microglia [23][24][25][26].

NEURODEGENERATION AND NEUROINFLAM-MATION
Neurodegeneration occurs when cells of central nervous system discontinue their physiological roles and eventually die, leading to a loss of neural function.It is mediated by the production of neurotoxic intermediaries, which activate inflammatory responses (neuroinflammation) [27].Neuroinflammation comprises the inflammatory response against abnormal proteins and their aggregates, pathogens and cell danger messengers, and the local activation of glial cells, astrocytes and oligodendrocytes leading to neuronal damage [27][28][29].1) is a schematic representation of the relationship between neurodegeneration and neuroinflammation.Alterations in cell metabolism and/or protein expression can lead to immune response activation.The migration of leukocytes to the CNS is a secondary event after local cell activation.
Pathogens and byproducts of cell death, as well as danger signals from damaged or stressed tissues (known as DAMPs), trigger the activation of local central nervous system cells through specialized pattern-recognition receptors (PRRs).Among the proteins involved in danger signals are heat shock proteins, chromatin, high mobility group box chromosomal protein 1 (HMGB-1), and aggregated modified or misfolded proteins such as amyloid-beta (Aβ), αsynuclein (α-syn), and tau.The main PRRs are the Toll-like receptors (TLRs) [29][30][31].However, other receptors are also involved in cell activation, such as advanced glycation endproducts receptors (RAGE) [32], VLDL/Apo E, and scavenger receptors that bind apolipoproteins lipoproteins and undegraded products of metabolic pathways (Fig. 2).Cell activation through these receptors leads to inflammasome activation (NLP3) along with Cas-1 generating IL1β and IL-18 through NFκB activation.NFκB activation induces the transcription of proinflammatory cytokines [31].The physiological inhibition of IL-1β is IL-1 receptor antagonist (IL-1ra) [33].This receptor binds IL-1β but does not generate a biological effect [33].In the absence of IL-1ra, the autocrine effects of IL-1β induce the transcription of IL-6 and TNFα, amplifying the inflammatory response.IFN α is produced  upon pathogenic infection and alerts the cells of pathogen invasion [34].IFNγ receptors are related to microglia activation in pathological conditions.Other cytokines like IL-17 can be produced by activated T lymphocytes recruited by the inflamed tissue, and this cytokine recruits neutrophils to the inflammatory site.
Inflammasome activation has been suggested to induce the onset of AD and PD [34].Senescence and inflammatory markers may help predict clinical progression in PD patients [35] since the innate immune sensors NLRP3 and Cas-1 are often activated [36].Dysregulated NLRP3 function observed in aged mice confirms the involvement of NLRP3 in cogni- tive dysfunction and physical performance; therefore, NLRP3 is an excellent therapeutic target for multiple agerelated neurological disorders [37].The IL-1β signal cascade is an essential pathogenic factor in NDs.Overexpression of caspase-1 and IL-1 β were reported in the nigrostriatal regions of a PD mouse model and the brain and cerebrospinal fluid of PD patients [38,39].Blocking IL-1β ameliorated pathological changes in a mouse model of AD [40].Even though evidence suggests that Caspase-1 may turn α-syn into a highly aggregation-prone variant [41], it is not directly responsible for the death of dopaminergic neurons.Unfortunately, Caspase-1 inhibitors did not improve the survival of grafted dopaminergic neurons in mouse PD models [42].Activation of TLR due to dysbiosis in the gut microbiome may further impair immunity and accelerate disease progression in PD patients [43].TLR gene transcription and protein expression are increased in NDs.TLR2 and TLR4 are upregulated in AD [44,45]; TLR2, TLR5 and CD14 in PD [28,46].It is yet unclear whether this over-expression is a compensatory mechanism against the accumulation of toxic proteins and/or alternative cell activation that contributes to disease progression [28,44], for example, the SNP Asp299Gly polymorphism of the TLR4 gene (linked to susceptibility to gram-negative bacterial infections) attenuates the inflammatory response.That specific polymorphism may protect against sporadic AD [45].
The accumulation of AGEs in cells and tissues is a standard feature of ageing, which is accelerated in neurodegeneration [32].AGEs are responsible for forming amyloid plaques and neurofibrillary tangles involved in astrocytosis, microgliosis, and neuronal cell death [32].Activated astrocytes, oligodendrocytes and microglia decrease myelin production and poorly execute repair mechanisms [47,48].NFkB plays an essential role in NDs since it is responsible for the transcription of proinflammatory cytokines [49,50].Several authors have reported an upregulation in the transcription of beta-amyloid precursor protein cleaving enzyme 1 (BACE1) by NFkB.BACE1 induces beta-amyloid production and the transcription of miR-125b in AD [48,49].Dopaminergic neurons in PD brains expressed higher levels of activated NF-κB than controls [50,51].Additionally, dysfunctional NFkB cell signalling is involved in neurodegeneration.NFkB promotes the transcription of proinflammatory cytokines [31] and high levels of RelA in the nigral dopamine neurons and glial cells.On the contrary, the c-Rel subunit can exert neuroprotective actions in PD [31].Uncontrolled TNF-α secretion plays a role in the pathogenesis of neurodegenerative disorders [52,53].TNF-related apoptosisinducing ligand (TRAIL) can be triggered in neurons by βamyloid and consequently cause apoptosis of brain cells [53].TRAIL is expressed in the cerebral cortex, often near Congo-red-positive amyloid plaques in the brains of AD patients [54].Cytokine accumulation in the brain has been observed in PD, ischemia, and AD, leading to chronic inflammation, gliosis, synaptic loss, and glutamate toxicity [55,56].In AD patients, increased pro-inflammatory cytokine levels are correlated with low levels of IL-1ra [56].It has become evident that acute inflammatory responses increase the risk and progression of neurodegenerative diseases; however, controlling inflammation and delivering suitable therapies on time can result in better patient outcomes.
The inflammatory response induces changes in BBB and BSCB, facilitating leukocyte migration.TLRs may also play roles in neuronal plasticity as they regulate the processes involved in neurogenesis and neurite outgrowth [24][25][26]48].Inflammaging is a state of chronic low-grade multi-organ inflammation often seen in older adults [59].Senescent cells, characterised by damaged or weakened cellular repair mechanisms, are responsible for this form of immune dysregulation.Most importantly, "pathogen-free" inflammation may contribute to PD and AD pathogenesis [60].Indirect evidence of subclinical inflammation was found in the Framingham study, where higher spontaneous production of IL-1 or TNFα (AD markers in older individuals) by peripheral blood mononuclear cells was observed and defined as subclinical inflammation [61].Under physiological conditions, α-syn, highly expressed in the brain, is involved in lipid metabolism, microtubule activity, modulation of tau phosphorylation and neurotransmitter release [62].In pathological circumstances, neurons can release α-syn, generating inflammatory responses.Impaired lysosomes cannot degrade internalised α-syn; thus, cathepsin B, a proteolytic enzyme that promotes inflammation [63], is released into the cytoplasm [63][64][65].Pathological α-syn becomes insoluble by forming βsheet-like oligomers (protofibrils) [66].This insoluble form interacts with microglial TLR2, which activates NF-κB and NLRP3, leading to the microglia's release of TNF-α and IL-1β, causing neuroinflammation in PD [67].This inflammatory cascade may be further exacerbated by mitochondrial dysfunction, observed in postmortem tissue of PD patients and models [68].A proposed mechanism for the progressive nature of PD is that misfolded oligomeric α-syn spreads from cell to cell and induces misfolding of native α-syn in a prionlike fashion [69], resulting in the loss of dopamine pathways in the substantia nigra (SN) and the development of Lewy bodies [69,70].Impaired dopamine activity is therefore responsible for slow movements (bradykinesia), muscular rigidity, trembling, postural instability, autonomous nervous system alteration and other nonmotor signs such as memory impairment [71].Increased secretion of abnormal proteins leads to the formation of autoantibodies.
Autophagy is impaired in NDs [72,73].The process is essential for cell survival and eliminating unwanted or pathogenic proteins and organelles.The critical sensor of the process is mTOR [72].In nourished neurons, phosphorylated mTOR blocks autophagy and apoptosis.However, mTOR can be anomalously activated in pathological stressed neurons by radicals, inflammatory intermediates and dysfunctional mitochondria, rendering cells unresponsive [72][73][74].Consequentially, cellular metabolic impairment in the CNS leads to neurodegeneration.Thus, metabolic impairment of cells in the CNS is responsible for several processes involved in neurodegeneration.
Several reports have linked lipid metabolism and transport genes with NDs [75].The involvement of APOE in AD has been extensively analysed.However, due to impaired mitochondria metabolism, lipid degradation is limited, promoting lipid accumulation in droplets.These lipid droplets lead to a more dysfunctional cell [76].Fatty acidoverloaded astrocytes accumulate acetyl CoA, inducing STAT3 activation [76].Activated STAT3 activates microglia and downregulates the production of cellular phospholipids and myelin [76].Dietary supplementation or regular consumption of healthy fats (ω3 fatty acids and short-chain fatty acids) seems to provide a certain degree of neuroprotection and reduce disease progression by lowering inflammation [77,78] and, perhaps, by improving the composition of the patient's microbiota [79][80].A genetic correlation between AD and gut microbiota has recently been published [81].In the analysis, Eubacterium fissicatena was found to be a protective bacteria, while Collinsella, and Veillonella species were linked to an increased risk.Further research is needed to establish the role of diet and microbiota in neurodegeneration and immune interactions.In the dopaminergic neurons of PD patients and mouse models, the microsomal enzyme prostaglandin E synthase-1 (mPGES-1) was shown to be overexpressed, and consequently, prostaglandin E2 levels were locally increased [75].Deleting the mPGES-1 gene stopped PGE2 production in these neurons and inhibited neurodegeneration in PD model 6-OHDA [75].Fig. ( 2) illustrates different cellular receptors and general responses related to neurodegeneration and neuroinflammation.On the left side, various receptors are essential in cell activation and stimulation of the immune response through cytokine secretion and abnormal proteins leading to autoantibody production.In the centre, the rest of the processes are described earlier.

IMMUNE RESPONSE IN NEURODEGENERATION
Microglia, a type of macrophage exclusive to the CNS, usually produces antiinflammatory molecules and neurotrophic factors (NF) that influence the behaviour of astrocytes and neurons [71].When these cells encounter pathogens or damaged tissue, they activate, promoting an inflammatory response that engages the immune system and initiates tissue repair.In most cases, this response is selflimiting.In ageing and other conditions such as AD, microglia become hyper-reactive, secreting large amounts of cytokines, chemokines, and other neurotoxic molecules.As expected, microglia have a different transcriptome profile in neurodegenerative diseases and ageing than normal tissue [35][36][37]82].Postmortem tissue from PD and AD patients exhibited HLA-DR + reactive microglia [38,39], which surges with neuronal degeneration throughout the nigrostriatal pathway in PD [39,40].
Astrocytes, microglia, and neurons express components of the complement pathway and its receptors [41], suggesting that local inflammation activates the complement cascade activation, leading to cellular stress and death.An increased amount of complement cascade molecules has been reported in the plasma, CSF, and brain tissues of patients with NDs [42]; for example, in PD patients, complement molecules are increased along with inflammatory cytokines [43].In AD, Aβ plaques are surrounded and infiltrated by activated astrocytes and microglia, which are believed to be the primary source of antigen-antibody-complement complex [83].
Fibrillar Aβ, β-pleated sheets, and tau neurofibrillary tangles have been shown to directly activate the classic complement pathway in vitro without antibodies [83].C1q was found to be tightly associated with Aβ plaques and caused surrounding neuronal atrophy through microglial engulfment [83].Additionally, C3 production was linked to increased activated NFκB in the brains of AD patients [83][84][85][86].Inhibition of the C1q pathway (using either antibody treatment or gene knockout) in wild-type mice prevented synapse loss after an injection of oligomeric-Aβ [85][86][87].Also, C5a receptor inhibitors seem to decrease Aβ plaque load and reduce hyperphosphorylated tau and neuroinflammation in AD mouse models [85,86].
Neutrophils are essential members of the innate immune response.They release proinflammatory and cytotoxic factors that induce cell death [88,89].They enhance cellular metabolism and cytokine-mediated signalling, organise mitochondria, and activate leukocytes in AD patients [89].These immune cells enter the AD brain via LFA-1 integrin and surround Aβ plaques with neutrophil extracellular traps (NET), promoting BBB damage and neuronal toxicity [89].In contrast, blocking LFA-1 integrin decreases neutrophil population and traffic in AD mouse models, reducing memory loss and neuropathological features [89].
Mast cells are tissue polymorphonuclear cells involved in innate immunity.They are involved in neuroinflammation by inducing oxidative stress, secreting chemokines and inflammatory cytokines, and activating microglia.These cells have been involved in AD and ALS [90].
NK cells are part of the innate immune lymphocytes (ILC) involved in the immunosurveillance of tumours and elimination of senescent cells [90].Their role in neurodegenerative disease is still under research.Its dysfunction is implicated in infection, malignancy, inflammatory disorders, and age-related senescent cell accumulation [91,92].Two NK cell subpopulations are detected in peripheral blood: a) A cytotoxic NK cell that expresses CD16 and is involved in neuroinflammation; b) A tolerogenic NK cell expressing CD56 and assisting in the resolution of neuroinflammation [92].NK cells have three main cytotoxic mechanisms: 1) the release of granzyme and perforin, 2) activation of the extrinsic apoptotic pathway by Fas ligand and TRAIL, and 3) antibody-dependent cell-mediated cytotoxicity (ADCC) [93,94].Alterations in peripheral NK cell number and receptor expression have been reported in PD patients and mouse models [94,95], yet additional research is needed to understand the role of these cells.

MHC and CD1 in Neuroinflammation
Different HLA genes associated with autoimmune diseases are linked to PD (HLA-DRA and HLA-DRB1) [18,19].HLA-DR antigens are upregulated in the microglia of these patients [96].Interestingly, a genome-wide association was observed between the CD1a gene polymorphism and the increase in neurofilament light in elderly individuals [97].Neurofilament light is a cytoplasmic protein highly expressed in large myelinated axons in neurological diseases.The migration of CD1a-positive myeloid cells into plaqueassociated microglia suggests a link between this antigen and neurodegenerative diseases.CD1a also presents T cells to self and abnormal lipids linked to AD [98].Dyslipidemia, inflammation and neurodegenerative diseases are connected; however, statin therapies have not been effective, at least in PD [99,100].
T cells that recognise Aβ1-42 as an antigen are detectable in AD [109] and likely contribute to forming plaques [110].AD patients had increased activated CD8+ T cells in the CSF compared to healthy older adults, correlating with clinical and structural AD markers [107].In AD, CNS infiltrating T cells produce IFN-γ and IL-17, activating microglia and exacerbating neuroinflammation [111][112][113][114]. CCL5 (RANTES) is the most common chemokine involved in AD neurodegeneration since it regulates the expression and secretion of normal T cells [111,115].
In murine models, upregulation of α-syn induces infiltration of B and T lymphocytes in the substantia nigra pars compacta [116][117][118] and CD3+/CD4+ T cell migration into the neocortex, hippocampus and striatum [117,118].However, dopaminergic neurons were spared if the mice were CD4 deficient [119].Lymphocyte-Activation Gene 3 (LAG3) Receptor (CD223) has been recently implicated in PD pathophysiology [120][121][122][123][124]. In a study performed in China, females were more likely to carry variants of this gene .Soluble CD223 was considered a prediction marker [123] since it interacts with TLR4, an essential trigger of neuroinflammation in PD [124,125].Even though CD223 is involved in Tcell inhibition and exhaustion, its role in PD remains a matter of research.
Transferring Tregs to reduce neuroinflammation and promote cell survival has been proposed as a therapeutic strategy for AD [133].Cognitive abilities improved in mouse models after treatment with Treg-blocked Th1 responses and reversed Aβ-induced inflammation [133].In turn, higher levels of IL-2, IL-6, TNFα, MCP-1 and T cells were found in PD models [125,128].
Moore and coworkers [134] showed that vitamin-D induction of T-reg cells in animal models decreased neurodegeneration.The therapeutic use of vitamin D in patients with neurodegenerative disorders has been proposed since many patients usually lack ergocalciferol [135].
Other T cytotoxic (Tc) subpopulations like Tc9 and Tc22 (Fig. 3) have been indirectly involved in mouse models of PD and AD; however, more studies are needed to define the role of these diseases and their importance in human pathology.
B cells may be directly involved in ND as they contribute to pathogenesis [140][141][142].Although B cells have not been detected in the brains of patients with PD [140,141], IgGcoating Lewy body [142] deposits are found on dopaminergic neurons, suggesting B cell activation is involved in this pathology.The amount of IgG immunopositive neurons is inversely proportional to the cell loss in the substantia nigra [142].Most neurons were IgG1-positive, but IgG2 and IgG3positive neurons were also present, IgG2 being mainly prominent in the damaged substantia nigra [142].
A general summary of the immune response observed in injuries and ageing is presented in Fig. (4).The figure aims to give a background of the changes in both conditions and how these changes can be related to NDs.Several characteristics observed in ageing are comparable to those described in NDs.

AUTOIMMUNITY MARKERS AND NEURO-DEGENERATIVE DISEASES
The presence of autoantibodies in NDs has been documented.Serum and CSF levels of antibodies against Aβ42 (the most aggregation-prone and neurotoxic species of Aβ) seem to differ between AD patients and healthy controls, but the research is inconsistent [143][144][145].Autoantibodies appear to be essential for AD diagnosis [146].
In an early study, autoantibodies against dopaminergic neurons were reported in the CSF of 78% of PD patients compared with 3% of controls [147].Chen et al. [148] demonstrated that plasma antibodies isolated from PD patients induced the loss of dopaminergic neurons in rats.Moreover, the CSF of PD patients showed a cytotoxic effect on dopaminergic neurons, which enhanced SN degeneration in a time-and dose-dependent manner [149].Multi-epitopic autoantibodies against α-syn were detected in the serum of 65% of all patients with PD [150]; their presence strongly correlated with an inherited mode of the disease but not other disease-related factors.In another study, total autoantibody levels were significantly higher in the PD group than in AD patients and healthy controls [151].Interestingly, one research group detected reduced α-syn natural autoantibody levels in patients with PD compared to individuals with AD and HC [152]; other groups have reported differences [153,154].Autoantibodies against melanin [155], GM1 ganglioside [156] and anti-beta2-glycoprotein I have also been described [157].There are several possible mechanisms by which autoantibodies may induce dopaminergic cell death [157]: 1) receptor-induced extrinsic apoptosis, 2) antibodycomplement complex cell death, 3) activation of surrounding microglia and 4) competitive binding inhibition [157].In 77 PD patients, Benkler et al. [158] found three prevalent autoantibodies: a) antineuronal cells 10.3% vs. 1.3% of controls; b) anti-brain lysate 9.1% vs. 1.3%; c) anti-dsDNA 10.3% vs. 2.6%.Anti-dsDNA was related to dyskinesia, whereas anti-dsDNA and anti-brain lysate were related to depression [158].Additionally, IgM autoantibodies and anti-myelinassociated glycoprotein (anti-MAG) were significantly elevated in the CSF of PD patients [158,159].It is imperative to mention that some autoantibodies have been observed in patients with para-neoplastic syndromes [160], although more research is needed to understand their presence better.
There is a molecular similarity between a protein of herpes simplex virus 1 (HSV1) and human α-syn [161]; autoreactive antibodies produced against HSV1 infection crossreact with a human α-syn homologous peptide.In a serologic study, 58% of PD patients were positive for this protein compared to 18% of controls [161].This peptide is expressed in the membrane of dopaminergic neurons, leading to immune cell attraction and activation, which later destroys them [161].
Antigenic epitopes can activate CD8 + T cells involved in autoimmune responses and may play an important role in neurodegenerative diseases [162].CD4+ and CD8+ T cells of PD patients recognise α-synuclein peptides [112,113,162], and genome-wide association studies have associated PD with MHC genes (HLA-DRA and HLA-DQB1) [18].Perhaps the thymus lacks α-syn epitopes, and thus, negative selection of T lymphocytes does not occur [163].
Neuromelanin (NM) is another potential target of autoimmune attacks on dopaminergic neurons as DC maturation is triggered upon their recognition [164].The autoimmune response against NM would be directed against NM-rich cells in the brain, leading to dopaminergic cell death [165].Unsurprisingly, PD patients were demonstrated to have higher levels of anti-neuromelanin antibodies in serum [164].Deposits of complement C1q on the surface of extracellular neuromelanin were found in the brains of postmortem PD patients [166,165].
Frontotemporal lobar degeneration (FTLD) is a neurodegenerative disorder characterised by intracellular accumulation of ALS-related proteins fused in sarcoma (FUS) and TAR DNA-binding protein 43 (TDP43), as well as tau.Behavioural alterations, language impairment, and deficits of executive functions are often observed in FTLD.Reports conclude that 23.4% of FTLD patients had serum autoantibodies against the GluA3 receptor, α-amino-3-hydroxy-5methyl-4-isoxazole propionic acid receptor (AMPAR) [167,168].The incubation of primary cultures of rat hippocampal neurons with anti-GluA3 antibody-containing CSF led to decreased GluA3 subunit synaptic localisation of the AMPA receptor and dendritic spine loss.Antibody titers correlate well with age at disease onset, with earlier symptom onset observed in those patients with higher antibody levels [167][168][169].One study observed autoantibodies in 18.9% of patients with degenerative dementia (FTD = 114, AD = 53, and -DLB = 7) [169].The autoantibodies most frequently detected were 1) the anti-extractable nuclear antibody profile, 2) the rheumatoid factor antibody, 3) the perinuclear antibody and 4) the cytoplasmic anti-neutrophil cytoplasmic antibodies [169].It is essential to mention that these antibodies are also usually involved in several autoimmune disorders.
AD considers Natural autoantibodies against Aβ protective since they assist protein clearance [186].However, active and passive immunisations with Aβ for therapeutic purposes may lead to immune-complex deposition and perivascular inflammation [186].
Autoantibodies to ATP synthase could be pathogenic in AD since they may inhibit ATP synthesis, alter mitochondrial homeostasis and induce apoptosis [184,187].In mice, the intracerebroventricular administration of ATP synthase autoantibodies, purified from AD patients, caused neuronal damage in the hippocampus [188].Also, autoantibodies to ceramide increased amyloid plaque burden in a transgenic mouse model of AD [189].Thus, using monoclonal antibodies to decrease the amount of abnormal protein deposition seems to produce pathologic precipitates in the tissue leading to more damage.

NEURODEGENERATIVE DISEASES IN PATIENTS SUFFERING AUTOIMMUNE DISEASES
The risk of neurodegenerative disease in patients with autoimmune diseases is still an area of intensive research.In Sweden, an analysis involving 310,522 patients and 33 autoimmune disorders showed an increased risk of PD in patients with Graves's disease, Hashimoto's disease, pernicious anaemia, and rheumatic polymyalgia [190].The same group reported a higher incidence of dementia in patients with type 1 diabetes mellitus, giant-cell arteritis, pernicious anaemia, Sjögren's syndrome, sarcoidosis, celiac disease, chronic rheumatic heart disease, Crohn's disease, chronic glomerulonephritis, pemphigus, psoriasis, rheumatoid arthritis, and ulcerative colitis [191].In a Korean population-based study, Cho et al. [192] showed that Graves' disease patients had a 33% higher risk of developing PD than controls, regardless of age, sex or comorbidities [192].However, one study did not find a significant difference in the prevalence of thyroid autoimmunity and dysfunction between PD patients and neurological controls (10.8% in PD patients vs. 10% in neurological controls) [193].These results were later confirmed in a meta-analysis [194].In a Mendelian randomisation study, multiple sclerosis and Sjögren syndrome were more strongly associated with AD than psoriasis, rheumatoid arthritis (RA) and type 1 diabetes [195].Epidemiological, genetic and clinical research is required on this topic.
There are still controversies concerning the possible risk of neurodegenerative diseases in patients with RA.Some groups have shown an increased risk of dementia [196][197][198], while others have not [199,200].On the other hand, Policicchio et al. [201] demonstrated a lower incidence of AD in RA patients [201].The discrepancies in interpretation may rely on the monitorisation of the inflammatory condition.Cooper and coworkers [202] showed a correlation between C reactive protein levels, RA and increased risk of PD [202], suggesting that chronic inflammation brought on by the disease may lead to the development of NDs.There is a higher prevalence of PD in patients with bullous pemphigoid, an autoimmune blistering dermatosis of elders, compared to patients with psoriasis [203].Further, patients with ankylosing spondylitis are at higher risk of AD and PD [204].
Inflammatory bowel disease, IBD (Crohn's disease and ulcerative colitis), was identified as an independent risk factor for PD and AD development [205][206][207].In a Danish study, IBD was associated with slightly increased dementia risk, particularly FTLD [205].Similar results were found in a Taiwanese study [206].One meta-analysis revealed a higher risk of AD and PD among Crohn's disease and ulcerative colitis patients [207].Another exciting report by Aggarwal et al. [208] showed that IDB patients manifested AD at younger ages and, in addition to IBD, other inflammatory poly arthropathies and systematic connective tissue disorders (psoriasis, rheumatoid arthritis and multiple sclerosis) are also linked to AD [209,210].In a Mendelian randomisation study, Cui and coworkers [210] found that individuals with IBD had a significantly higher risk of developing PD.However, other Mendelian randomisation studies showed no evidence of an association between IBD and PD [211,212].There are still many questions to answer on this topic, as research is quite contradictory.
In Taiwan, Lui FC and coworkers [213] reported an inverse association between systemic lupus erythematosus (SLE), a chronic, systemic autoimmune disease, and the risk of PD, with the crude hazard ratio (HR) being 0.60 (95% confidence interval 0.45-0.79) in comparison with non-SLE patients in a population-based study.Nonetheless, systemic lupus erythematosus and Sjögren syndrome were highly associated with dementia risk in a study by Wang and coworkers [214].Yet, there wasn't a significant causal association between SLE and AD in another Mendelian randomisation study [215].
The association between autoimmunity and neurodegenerative diseases is still an evolving topic.In the next section, the effect of therapies that modulate the immune response in autoimmune diseases has generated new perspectives which are essential to analyse.

IMMUNOLOGIC TREATMENT AND RISK OF NEURODEGENERATIVE DISEASE
In animal models of PD, a reduction in dopaminergic neuron degeneration has been observed in animals treated with nonsteroidal antiinflammatory drugs (NSAIDs) [216].In two prospective studies (men Health Professionals Follow-up Study,1986-2000, and Women Nurses' Health Study, 1980-1998), a lower risk (0.55) of PD onset was found in the participants who reported regular use of nonaspirin NSAIDs as compared to the non-regular users [217].In addition, a lower, but not highly significant, risk of PD was also observed among men and women who took two or more aspirin tablets daily compared with nonusers [217,218].In another cohort of men and women from the US (The Cancer Prevention Study II Nutrition Cohort), PD risk was lower among ibuprofen users than nonusers [219].Compared with nonusers, the relative risks were 0.73% for people who consumed fewer than two tablets/per week and 0.62% for those who had one or more tablets/per day [216][217][218].Gao and coworkers [219] reported an association between ibuprofen and lower PD risk, not shared by other NSAIDs or acetaminophen.In another study (Neuro Genetics Research Consortium), smoking, coffee, and over-the-counter NSAID use as individual factors exhibited a 20% to 30% risk reduction for PD [220].Multi-analysis associated the leucine-rich repeat kinase--2 gene penetrance with NSAID use and PD [221].However, recent meta-analyses had contrasting results for the same disease [222,223].Table 1 illustrates the effect of different compounds with anti-inflammatory effects.
Patients with RA treated with TNF-blocking agents (etanercept, adalimumab, infliximab) rarely develop AD [224,225].In addition, TNF inhibitors showed a long-term effect in reducing the risk of AD during 20 years of followup in RA patients [226].On the other hand, Etanercept and Adalimumab were associated with lower AD risk in patients with psoriasis [225,226].Methotrexate may also have neuroprotective effects [227].Similarly, the benefit of anti-TNF therapy was observed in patients with ankylosing spondylitis [228].On the contrary, no effect was seen in patients using conventional disease-modifying antirheumatic drugs (cDMARD) [228].One study reported a 78% reduction in the incidence rate of PD among patients with inflammatory bowel disease exposed to anti-TNF therapy compared with those not [229].
A lower risk for AD was also associated with using methotrexate combined with anti-TNF [230].Although, there was no significant difference comparing the risk of AD between RA patients receiving Methotrexate or TNF blockers, only a combination of both [230].Treatment with abatacept (T-cell activation inhibitor) plus tofacitinib (JAK inhibitor) and tocilizumab (IL-6 inhibitor), or TNF inhibitors, did not decrease the risk of AD in arthritic patients [231].Studies revealed no statistical association between Alzheimer's disease and hydroxychloroquine use [232,233].A recent publication showed the contrary, with a lower AD incidence risk than methotrexate [234].Other immunemodulating drugs like sulfasalazine have been linked to neuropathic pain and migraine but not dementia [235].Further evidence is required.
A decreased incidence of AD has also been observed with other treatments used in autoimmune diseases.Patients treated with calcineurin inhibitors who underwent a solid organ transplant have a lower incidence of AD than the general population [238].Diagnoses of AD were reduced among individuals ≥ 65 years with prior influenza vaccination compared to those without the vaccine [239].In a group of patients with bladder tumours, age ≥ 75 years, those treated with intravesical Bacillus Calmette-Guerin (BCG) had a significantly decreased risk of developing AD and PD as compared to patients who only underwent transurethral resection [240].Other drugs like metformin are still under discussion [241].Epidemiological analysis of large-scale populations may provide more associations since the above publications could only represent random and unspecific associations when large trials or studies are conducted.

IMMUNOPHARMACOLOGY AND NEURODEGE-NERATIVE DISEASES
Studies on inflammation, autoimmunity, and neurodegenerative diseases have opened new therapeutic options in neurodegenerative diseases.In vitro, releasing toxic factors by activated microglia can be partially blocked by NSAIDs [242].
To facilitate the analysis of different strategies that have been used in PD and AD, we divided the most relevant ones into tables.Table 1  represents tested antiinflammatory compounds, mainly in animal models.The analysis of NSAID, as commented before, was tested in two clinical trials in which no reports have been published suggesting its lack of effect on AD.It should be noted that the population study involved normal individuals in which the risk of NDs was analysed over time compared with the drug's effect on individuals with the incipient disease.The use of antitumour drugs is exciting since it may provide new options for patients with known genetic risks for the disease.The rest of the compounds have not reached clinical trials, but chemical modifications may lead to exciting structures with potential use in NDs.
A fascinating approach based on different populations' diets and natural remedies has identified several natural compounds.The primary goal is to decrease oxygen and nitrogen radical formation and discover new anti-inflammatory structures that could pass the blood-brain barrier.Oral intake of some of these compounds has been proven to reduce ND onset and progression.Most of these compounds are flavonoids that significantly affect immune response in several diseases [278].
Different structures used to treat various diseases were repurposed for NDs.Three critical pathways were targeted: NLP3/Cas-1, TNFα inhibition, immunomodulation, p38αMK2 and the aryl hydrocarbon receptor (Table 1).Promising compounds in preclinical studies underwent clinical trials with Small synthetic molecules Inhibits p38α and axis MK2 AD/PD Yes Not yet [277] mixed results.Neflamapimod seems to be the most promising compound, although more clinical trials and long-term follow-up are required [273,274].Laniquimod was previously used to treat MS, is now used to treat HD and may have a significant role in synucleinopathies by decreasing neuroinflammation [275].Table 2 illustrates the effect of different natural products tested in AD and PD, Curcumin also seems to activate the aryl hydrocarbon receptor, reducing neuroinflammation [309].
As described earlier, complement is produced by different cells in the CNS and autoantibodies against the abnormal pro-teins have been detected [309].Therefore, cell death due to antibody complement complex can be blocked by know inhibitors.Even though results in animal models seem promising, there has been only one clinical trial involving neuromyelitis optica, and no other trials have been proposed.This therapy may be used in combination with others as a coadjuvant.
The use of cytokine inhibitors in NDs is an exciting approach (Table 3); however, the main problem is treating patients with symptoms, especially during the early phases.TNFα inhibitors, also used in autoimmune diseases, have been reported the most.The use of other inhibitors is still   Secondary effects?[345][346][347] under scrutiny (Table 3).Inhibitors of other cytokines, IL-1 receptor antagonists and IL-12/IL-23 have been analyzed (Table 3).The possible role of IL-10 is under discussion [326].
Anti-Aβ antibodies in healthy individuals were the basis for clinical trials of intravenous immunoglobulin (IVIg) in patients with AD.However, despite promising initial results, a recent meta-analysis of blood derivatives showed no clear benefit of IVIg after five clinical trials despite promising initial results [327].No current clinical trials involve IVIg in neurodegeneration.
The use of monoclonal antibodies in AD has gained attention in recent years.After the lack of effect of the first monoclonals, several new schemes for generating new antibodies were used (Table 4).The more successful ones are Aducanumab and Lecanemab, two antibodies approved by the FDA for AD.Aducanumab has not significantly improved cognitive response in AD patients (Table 4).Nevertheless, there have severe concerns with Lecanemab about brain shrinkage and patient death.This high-affinity antibody can probably activate damaged cell death, decreasing brain volume [348].It may be helpful to analyse brain autopsies in detail and the mechanism of this effect before discontinuing their use in the clinic.
Considering that autoantibodies are usually produced against abnormal or phosphorylated tau, it is an excellent strategy to immunize against abnormal tau to prevent the effect of this protein on healthy tissues (Table 5).The vaccine would require the activation of specific non-polyclonal B cells.It is still early to analyze the first vaccine's impact; nonetheless, several other vaccines are underway, which may be interesting to compare.The use of monoclonal antibody therapies against α synuclein has not been, up to date, thriving despite the different types of antibodies generated against the variety of pathological proteins (Table 6).Moreover, vaccine trials are still underway, and it is too early to state whether they are effective (Table 7).

OTHER TREATMENTS
Treatments with cytokines that downmodulate inflammatory cytokines and cell activation have also been proposed.One example is the granulocyte-macrophage colonystimulating factor (GM-CSF).In the PD mouse model, GM-CSF treatment generated a protective Treg response by downregulating microglial activation and decreasing the death of dopaminergic neurons [381].Sargramostim (GM-CSF) demonstrated a safe and well-tolerated profile.In phase I clinical trials with PD patients, NCT03790670 sargramostim increased Treg frequencies and function without affecting the levels of effector T cells [381].Compared with pretreatment baselines and placebo-treated controls, sargramostimtreated patients had lower clinical ratings of disease severity, and magnetoencephalography revealed improved signalling in cortical regions relevant to motor function [382].Five patients with Parkinson's disease who were administered sargramostim for a duration of one year experienced a reduction in Movement Disorder Society-Sponsored Revision of the Unified Parkinson's Disease Rating Scale (MDS-UPDRS) scores [383].A new clinical trial, NCT05677633, on biomarker validation following sargramostim treatment is underway.
Therapeutic plasma exchange (TPE) plasmapheresis reduces the concentration of pathology-related contents in plasma.TPE has been used in AD [384] and may benefit patients by an entirely different mechanism, potentially opening a new avenue for future research [385].A phase 2b/3 Alzheimer's Management by Albumin Replacement   (AMBAR) study shows that TPE with albumin exchange may slow cognitive and functional decline in AD patients [385].A significant improvement in quality of life was measured by a self-reported questionnaire among patients with mild AD from baseline to 14 months among the TPEtreated groups compared with the control group.There are still several areas in this topic that require more research.
Among other strategies proposed is using small molecules to target checkpoint receptors in neuroinflammatory diseases [386].Also, the inhibition of the pathway IL-17/TRAF6 as this pathway is involved in neurotoxicity [387].Finally, the use of therapies to expand Treg cells seem to be important not only in MS but also in PD [388].The development of new treatments is just beginning.

CONCLUSION
Various schemes involving AD and PD have been used to control acute and/or chronic inflammatory responses to decrease the risk or slow the progression of neurodegenerative diseases.In both diseases, there is still room for im-provement.Several therapies for autoimmune diseases have been proven helpful in the onset or progression of NDs.Several anticancer drugs may be beneficial, as in the case of methotrexate in rheumatoid arthritis.The critical issue is assessing the risk and diagnosing the condition in time to start with good therapeutic schemes involving balanced nutrition, supplementation, and physical and cognitive exercises (https://www.alz.org/alzheimers-dementia/treatments/alternative-treatments). Genetic counselling of families of patients with NDs may help identify those with higher genetic risk and provide alternatives to delay disease onset.
Currently, safe therapeutic options involve cytokine inhibitors and other anti-inflammatories in patients with stable disease or typical progression.Monoclonal antibodies against βA must be closely monitored due to their adverse effect.
In patients with rapid progression, there is no primary option available.However, clinical trials should consider this group as more people develop NDs at younger ages.
Reducing inflammation with an array of early-stage treatments is the most promising strategy to mitigate the development of underlying AD and PD pathophysiology [356].There is, however, room for improvement in pathological screening and the generation of new therapeutic compounds, as well as strategies and schemes that can benefit these highly prevalent diseases.

Fig. (
Fig. (1) is a schematic representation of the relationship between neurodegeneration and neuroinflammation.Alterations in cell metabolism and/or protein expression can lead to immune response activation.The migration of leukocytes to the CNS is a secondary event after local cell activation.

Fig. ( 1
Fig. (1).General overview of the interaction between neurodegenerative diseases, immune response, neuroinflammation and neurodegeneration.On the left side, ageing, genetic and epigenetic factors, and viral, microbial or parasite infections induce alterations in cell metabolism with impaired abnormal protein degradation, autophagy and apoptosis, and the secretion of pathogenic proteins (red arrow).Pathogenic proteins can induce neurodegeneration and immune response activation (red arrows).All the previous events can cause activation of the immune response (purple arrow).Local and/or peripheral immune response activation induces neuroinflammation (brown arrow), leading to neurodegeneration.Neural cell death also activates the immune response (red double arrows).(A higher resolution/colour version of this figure is available in the electronic copy of the article).

Fig. ( 2 ).
Fig. (2).The cellular receptors and pathways involved in neurodegeneration and neuroinflammation.The figure represents the events involved in cell activation in CNS.The processes of cell activation englobe microglia, oligodendrocytes, astrocytes and neurons.(A higher resolution/colour version of this figure is available in the electronic copy of the article).

Fig. ( 3 )
Fig. (3).Illustrates the diverse components of the immune response involved in neuroinflammation.(A) Three groups are observed.The innate immune response group involves microglia, mastocytes, neutrophils, macrophages, dendritic cells and proteins of the complement cascade.The second group, with innate and adaptative immune response characteristics, are NK, NKT and Tγδ cells.The adaptative group included T lymphocytes, B lymphocytes, antibodies and cytokines.(B) illustrates the major T-cell subpopulations that arise depending on the central CD4 and CD8 subpopulation, the antigen presented and the cytokines involved in the differentiation.Cytokines are crucial for the differentiation of T-cell subpopulations, which are involved in physiological and pathological responses.(A higher resolution/colour version of this figure is available in the electronic copy of the article).

Fig. ( 3
Fig. (3) depicts the different subpopulations that arise from naïve CD4 and CD8 cells, the cytokine requirements and the production of cytokines.The role of the different

Fig ( 4 )
Fig (4).The schematic figure illustrates the main characteristics of immune response in injuries, infection and ageing in the CNS.

FUNDING
This review was supported by The Grant Agency of the Czech Republic responsible Dr V Das (23-06301J).This review was supported by infrastructural projects (CZ-OPENSCREEN -LM2023052; EATRIS-CZ -LM2023053), the projects National Institute for Cancer Research (Project No. LX22NPO5102), National Institute for Neurological Research (Project No. LX22NPO5107), National Institute of virology and bacteriology (Programme EXCE LES, ID Project No. LX22NPO5103) -Funded by the European Union -Next Generation EU from the Ministry of Education, Youth and Sports of the Czech Republic (MEYS)) and PerMed Personalised Medicine: From Translational Research into Biomedical Applications project number TN02000109.